Sandbox:Sogand: Difference between revisions

Latest revision as of 22:34, 5 October 2020


jhfdjg


Anemia

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Sogand Goudarzi, MD [2]

Abnormal hematosis


past history	imaging finding
Past medical history was unremarkable	coronory angiography	intracoronary imaging	CTCA
Past medical history was unremarkable

syndrome


Staging for mycosis fungoides and Sezary syndrome
Skin (T)
T1	Limited patches, papules, and/or plaques covering <10% of the skin surface. May further stratify into T1a (patch only) versus T1b (plaque patch)
T2	Patches, papules, or plaques covering 10% of the skin surface. May further stratify into T2a (patch only) versus T2b (plaque patch).
T3	One or more tumours (1-cm diameter)
T4	Confluence of erythema covering 80% body surface area
Node (N)
N0	No clinically abnormal peripheral lymph nodes; biopsy not required
N1	Clinically abnormal lymph nodes; histopathology Dutch grade 1 or NCI LN0-2
N1a	Clone negative
N1b	Clone posetive
N2	Clinically abnormal peripheral lymph nodes; histopathology Dutch grade 2 or NCI LN3
N2a	Clone negatove
N2b	Clone posetive
N3	Clinically abnormal peripheral lymph nodes; histopathology Dutch grades 3e4 or NCI LN4; clone positive or negative
NX	Clinically abnormal peripheral lymph nodes; no histologic confirmation
Visceral (M)
M0	No visceral organ involvement
M1	Visceral involvement (must have pathology confirmation and organ involved should be specified)
Blood (B)
B0	0 Absence of significant blood involvement: 5% of peripheral blood lymphocytes are atypical (Sezary) cells B0a Clone negative B0b Clone positive
B1	Low blood tumour burden: >5% of peripheral blood lymphocytes are atypical (Sezary) cells but does not meet the criteria of B2 B1a Clone negative B1b Clone positive
B2	High blood tumour burden: 1000/mL Sezary cells with positive clone

T

Mycosis fungoides

Stage IA-IIA

Stage IIA

Stage III

Stage IV

• Expectane policy
• Topical steroides [IV-A]
• nb-UVB[III,A]
• PUVA [III-A]
• Topical mechlorethamine [II,B]
• Local RT [IV,A]

• Skin direct therapy(SDT) + local radiotherapy
• ST[III+A]
• (SDT+) retiods[III,B]
• (SDT+) IFN a {III,B]
• TSEBT [III,A]

• (SDT+) retinoides
• (SDT+) IFNa
• ECPI INFa +/- rtinoides
• Low dose MTX
• [IV-B]

• Gemcitabine
• Liposomal doxorubicin
• Brentuximab vedotin[II,B]

• (SDT+) retinoides [III,B]
• (SDT+) IFNa [III,B]
• Retinoides +IFN a [II,B]
• TSEBT [IV,A]

• Gemcitabin [IV,B]
• Liposomal doxorubicin [IV,B]
• Brentuximabvedotin [II,B]
• Combinatio Cht [Iv,B]
• AlloSCT[V,C]

TSEBT[LV,B]

• Combination Cht [IV,B]
• AlloSCT [V,C]

Differentiating [disease name] from other diseases on the basis of [symptom 1], [symptom 2], and [symptom 3]

On the basis [symptom 1], [symptom 2], and [symptom 3], [disease name] must be differentiated from disseminated intravascular coagulation (DIC) , thrombotic thrombocytopenic purpura (TTP),systemic vasculitis , [disease 4], [disease 5], and [disease 6].

	Symptoms			Physical examination				Lab Findings												Occur			Histopathology
Diseases	Clinical manifestations							Para-clinical findings																Gold standard	Additional findings
	Symptoms			Physical examination				Para-clinical findings
	Diarrhea	Abdominal pain	decrease urin	Physical exam 1	Physical exam 2	fd	CBC	PC	PT	PTT	FDP	D-dimer	LDH	haptoglobin	Coombs test	PBS	BUN	Cr	S/C	Pediatric	Adult	Imaging 3	Histopathology
Disseminated intravascular coagulation (DIC)								NL/_	↑	↑	↑	↑
Hemolytic uremic syndrome							Hemolitic anemia		NL	NL	NL	↑	↑	↑			↑	↑		+++	+
Thrombotic thrombocytopenic purpura (TTP)																				+	+++
Systemic vasculitis
Diseases	Symptom 1	Symptom 2	Symptom 3	Physical exam 1	D	Physical exam 3		Lab 1	Lab 2	Lab 3										Imaging 1	Imaging 2	Imaging 3	Histopathology	Gold standard	Additional findings
Differential Diagnosis 4
Differential Diagnosis 5
Differential Diagnosis 6

References

Differentiating between Hemoglobinopathies


		Gene type	Red blood cell (RBC) count g/dl			Hemoglobin pattern	Differentiating Symptoms
		Gene type	Hemoglobin g/dl	MCH /pg	Hemoglobinpattern	Hemoglobin pattern	Differentiating Symptoms
Alpha Thalassemia		-+/++	Normal	Normal	Normal	Normal	None
		-+/-+ --/++	Normal or low	<26	Normal	Normal	Mild anemia
		--/-+	8 to 10	<22	HbH &asymp 10 to 20%	HbH 10 to 20%	Chronic hemolytic anemia
		Hb Bart’s hydrops fetalis --/--	<6	<20	Hb Bart’s 80 to 90%, Hb Portland ≈ 10 to 20%, HbH <1%	Hb Bart’s 80 to 90%, Hb Portland 10 to 20%, HbH <1%	Life-threatening fetal anemia
β-thalassemia	Heterozygous	&β/++	9 to 15		HbA2 >3.2%
		&β/+-			HbF 0.5 to 6%
		&β/--		19 to 25
	Compound heterozygous	β + /β 0
	Homozygous	β+/β+	<7
		β 0 /β 0

Sickle cell Disease			6 to 9
HBC

Pathophysiology

The pathophysiolgy of xxx disease in unknown.
But it may follow xxx pathway

- It is believed that xxx might work on yyy to produce zz.

Pathology

Idiopathic
Itarogenic
cardiac

References

History & clinical symptoms

Blood test

hemolysate

Diagnosis of abnormal hemoglobins

Diagnisis of β-thalassemia

Dignisis of α-thalassemia

Alkaline electrophoresis
• acid electrophoresis
•HPLC

Electrophoresis HPLC
• HbA2,Hbf

Electrophoresis HPLC
• DNA testing

Evidence of abnormality,comparison of mobility with that of known abnormalities, if HBS suspected: solubility test

Separation/quantification

Evalution of all data and findings

Diagnisis of β-thalassemia

Dignisis of α-thalassemia

DNA sequencing if needed

DNA sequencing if needed(thalassemia major, thalassemia intermedia

Evaluation of all data and findings(including blood count ethnic and origin

Diagnosis of hemoglobinopathy

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 __NOTOC__
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+! colspan="4" |jhfdjg
+|-
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+|}
 <br />
 {| class="wikitable"
@@ Line 65: / Line 81: @@
 | rowspan="2" |
 | rowspan="2" |
-| rowspan="2" |Past medical history was unremarkable
+| rowspan="2" |Past [[medical]] history was unremarkable
 |coronory angiography
 |intracoronary imaging
@@ Line 83: / Line 99: @@
+[[syndrome]]
 {| class="wikitable"
 |+
 ! colspan="3" style="background: #4479BA; color: #FFFFFF; text-align: center;" |Staging for mycosis fungoides and Sezary syndrome
 |-
 ! colspan="3" style="background: #B0C4DE; color: #FFFFFF; text-align: center;" |'''[[Skin]] (T)'''
@@ Line 133: / Line 149: @@
 |[[Clinical|Clinically]] [[abnormal]] [[T-cell lymphoma classification|peripheral]] [[Lymph node|lymph nodes]]; no [[histologic]] confirmation
 |-
-! colspan="3" style="background: #B0C4DE; color: #FFFFFF; text-align: center;" |[[Visceral|'''Visceral''']] ('''M''')
+! colspan="3" style="background: #B0C4DE; color: #FFFFFF; text-align: center;" |'''[[Visceral|Visceral]]''' ('''M''')
 |-
 | align="center" style="background:#ADD8E6;" |M0
@@ Line 141: / Line 157: @@
 |[[Visceral]] involvement (must have [[pathology]] confirmation and [[Organ (anatomy)|organ]] involved should be specified)
 |-
-! colspan="3" style="background: #B0C4DE; color: #FFFFFF; text-align: center;" |[[Blood|'''Blood''']] '''(B)'''
+! colspan="3" style="background: #B0C4DE; color: #FFFFFF; text-align: center;" |'''[[Blood|Blood]]''' '''(B)'''
 |-
 | align="center" style="background:#ADD8E6;" |B0
@@ Line 169: / Line 185: @@
 {{familytree | | | D01 | | D02 | | | D03 | | | D04 | | |D01=<br>• (SDT+) retinoides [III,B] <br>• (SDT+) IFNa [III,B] <br>• Retinoides +IFN a [II,B] <br>• TSEBT [IV,A] |D02=<br>• Gemcitabin [IV,B] <br>• Liposomal doxorubicin [IV,B] <br>• Brentuximabvedotin [II,B] <br>• Combinatio Cht [Iv,B] <br>• AlloSCT[V,C] |D03=TSEBT[LV,B] |D04=<br>• Combination Cht [IV,B] <br>• AlloSCT [V,C] | | |}}
 {{Family tree/end}}
@@ Line 264: / Line 279: @@
 ![[haptoglobin]]
 ![[Coombs test]]
 !PBS
 !BUN
 !Cr
@@ Line 285: / Line 300: @@
 |'''↑'''
 |'''↑'''
-|  '''↑'''
+|'''↑'''
-|  '''↑'''
+|'''↑'''
 |
 |
@@ Line 508: / Line 523: @@
 ==References==
-== Differentiating between Hemoglobinopathies ==
+==Differentiating between Hemoglobinopathies==
 {| class="wikitable"
@@ Line 533: / Line 548: @@
 --/++
 |Normal or low
 |<26
 | colspan="2" |Normal
 |Normal
@@ Line 539: / Line 554: @@
 |-
 | --/-+
 |8 to 10
 |<22
 | colspan="2" |HbH &asymp
 to 20%
@@ Line 549: / Line 564: @@
 --/--
 |<6
 |<20
 | colspan="2" |
-* Hb Bart’s 80 to 90%,
+*Hb Bart’s 80 to 90%,
-* Hb Portland &amp;asymp; 10 to 20%,
+*Hb Portland &amp;asymp; 10 to 20%,
-* HbH <1%
+*HbH <1%
 |Hb Bart’s 80 to 90%,
 Hb Portland 10 to 20%,
@@ Line 563: / Line 578: @@
 | colspan="3" rowspan="3" |Heterozygous
 |&β'''/'''++
 |9 to 15
 |
 | colspan="2" |HbA2 >3.2%
@@ Line 643: / Line 658: @@
 ==Pathophysiology==
-# The pathophysiolgy of xxx disease in unknown.<ref name="WellsPacini2013">{{cite journal|last1=Wells|first1=Samuel A.|last2=Pacini|first2=Furio|last3=Robinson|first3=Bruce G.|last4=Santoro|first4=Massimo|title=Multiple Endocrine Neoplasia Type 2 and Familial Medullary Thyroid Carcinoma: An Update|journal=The Journal of Clinical Endocrinology & Metabolism|volume=98|issue=8|year=2013|pages=3149–3164|issn=0021-972X|doi=10.1210/jc.2013-1204}}</ref>
-# But it may follow xxx pathway
+#The pathophysiolgy of xxx disease in unknown.
-#*It is believed that xxx might work on yyy to produce zz.<ref name="pmid21819630">{{cite journal |vauthors=Boujelbene N, Cosinschi A, Boujelbene N, Khanfir K, Bhagwati S, Herrmann E, Mirimanoff RO, Ozsahin M, Zouhair A |title=Pure seminoma: a review and update |journal=Radiat Oncol |volume=6 |issue= |pages=90 |date=August 2011 |pmid=21819630 |pmc=3163197 |doi=10.1186/1748-717X-6-90 |url=}}</ref>
+#But it may follow xxx pathway
+#*It is believed that xxx might work on yyy to produce zz.
 ===Pathology===
 *Idiopathic
 *Itarogenic
@@ Line 673: / Line 692: @@
 == References ==
+<references />

Sandbox:Sogand: Difference between revisions

Latest revision as of 22:34, 5 October 2020

Abnormal hematosis

Differentiating [disease name] from other diseases on the basis of [symptom 1], [symptom 2], and [symptom 3]

References

Differentiating between Hemoglobinopathies

Pathophysiology

Pathology

References

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